SBRT Clinical Trial
Official title:
Stereotactic Hypofractionated Accelerated Radiotherapy Post-Prostatectomy: a Phase I Feasibility Study
The present phase I trial evaluates the feasibility of a postoperative stereotactic
hypofractionated external beam radiation therapy delivered in patients who underwent radical
prostatectomy with adverse pathological features or early biochemical failure. Modern
computer-driven technology enables the implementation of ultra-high hypofractionated
Image-Guided Radiotherapy (IGRT) safely.
Eligible patients for this study are those with:
- Adenocarcinoma of the prostate treated with radical prostatectomy (any type of radical
prostatectomy is permitted including retropubic, perineal, laparoscopic or robotically
assisted; there is no time limit for the date of radical prostatectomy)
- Pathologic (p)T3 disease, positive margin(s), Gleason score 8-10, or seminal vesicle
involvement
- Undetectable post-radical prostatectomy PSA that becomes detectable and then increases
on 2 subsequent measurements (PSA of > 0.1 - ≤ 2.0 ng/mL)
- Life expectancy: 10 years
- ECOG performance status of 0 -1
- No distant metastases, based on the following workup within 60 days prior to
registration
- Magnetic resonance imaging (MRI) of the pelvis
- PSMA/Choline Positron Emission Tomography (PET) to exclude systemic disease in patients
with biochemical recurrence
- Patients can be on androgen deprivation therapy
- Ability to understand and willingness to sign a study-specific informed consent prior to
study.
Patients enrolled in the study will undergo image-guided, volumetric intensity-modulated arc
radiotherapy (IGRT-VMAT) with state-of-the-art treatment-planning and quality assurance
procedures with emphasis on normal tissue sparing and delivery accuracy via the use of
devices that ensure stability and beam location reproducibility.
The present study evaluates the feasibility of postoperative stereotactic hypofractionated
external beam radiation therapy delivered in patients who underwent radical prostatectomy
with adverse pathological features or early biochemical failure. Regardless the two settings
(adjuvant or salvage), external beam radiation therapy for prostate cancer is usually a
protracted course, since a total dose of 66 Gy to 70 Gy is needed to be effective. At the
typical rate of 1.8 Gy to 2.0 Gy per treatment, it takes approximately 35 treatments over the
course of 7 weeks to complete, which is very costly and extremely time consuming. On the
other hand, the α/β ratio for prostate cancer has estimated to be as low as 1.5 Gy,
significantly lower than the 3 Gy value estimated for late complications.Therefore, the
delivery of the same equivalent total dose at 2 Gy/fraction (normalized total dose) to the
prostate using a hypofractionation regimen, a part from the practical benefits of reducing
the treatment cost and number of sessions for patients to radiotherapy departments, should
have a sparing effect on early responding normal tissues through the reduction in the total
dose delivered, as well as a reduction in the incidence of late complications. Trials
investigating clinical and toxicity outcomes of moderate hypofractionation schedules in the
curative setting have reached sufficient follow-up to show similar efficacy and toxicity to
conventionally fractionated regimens.
Stereotactic body radiation therapy, or SBRT, is on the shortest end of the hypofractionation
spectrum. It is accomplished in a five treatments. With its pinpoint accuracy, many
Institutions currently use it for primary treatment at doses up to 9 Gy per treatment,
leading to excellent outcomes at least at early time points.Patients enrolled in the study
will undergo image-guided, volumetric intensity-modulated arc radiotherapy (IGRT-VMAT) with
state-of-the-art treatment-planning and quality assurance procedures with emphasis on normal
tissue sparing and delivery accuracy via the use of devices that ensure stability and beam
location reproducibility.A rectal balloon with air filling will be used for anatomical
reproducibility, while a urethral catheter loaded with beacon transponders will be used to
ensure set-up reproducibility and online target tracking. Previously untreated patients who
underwent radical prostatectomy with adverse pathologic findings will be enrolled in a phase
I study, consisting of 31 Gy (5 fractions of 6.2 Gy), respectively, delivered over a 1-week
period at 5 fractions per week. This dosage corresponds to 68.2 Gy (for an α/βratio estimate
of 1.5 Gy), compared to 52.7 Gy (for an α/β estimate of 4 Gy) in a conventional schedule. In
those who developed early biochemical failure the radiation schedule will consists in 32.5 Gy
(5 fractions of 6.5 Gy), respectively, delivered over a 1-week period at 5 fractions per
week. This dosage corresponds to 74.3 Gy (for an α/β ratio estimate of 1.5 Gy), compared to
56.9 Gy (for an α/β estimate of 4 Gy) in a conventional schedule.
Patients will be followed at one month post-treatment and every 3 months for up to 12 months
(+/- 4 weeks) and every 6 months thereafter. Acute and chronic toxicity evaluations will
focus, though not exclusively, on urinary, rectal and sexual functions and will be assessed
through validated EPIC questionnaires. Serum PSA values will be drawn on the same schedule as
clinical follow-up. The study will be continuously monitored for a minimum of 5 years. In the
event unexpected severe (grade ≥3) toxicities are observed in any one of the treatment
regimens, the trial will be terminated according to the standard stopping rules: >3/first 10,
and >5/first 25 patients.
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